AJP - Regulatory, Integrative and Comparative Physiology, Vol 264, Issue 5 1004-R1009, Copyright © 1993 by American Physiological Society
Peroxisomal beta-oxidation is a significant pathway for catabolism of fatty acids in a marine teleost
E. L. Crockett and B. D. Sidell
Department of Zoology, University of Maine, Orono 04469.
Hepatic beta-oxidation is characterized in a marine teleost, Myoxocephalus
octodecimspinosus, to determine mitochondrial and peroxisomal substrate
selectivity as well as metabolic partitioning. Substrate selectivity is
broad for peroxisomal beta-oxidation. Acyl CoA oxidase activities, with all
unsaturated substrates measured, are at least 35% of activity with
palmitoyl CoA (16:0), a saturated substrate. Mitochondrial selectivities
are more pronounced. Carnitine palmitoyltransferase activity with a
monounsaturate, palmitoleoyl CoA (16:1), is nearly 40% greater than
activity with palmitoyl CoA, whereas activities with two polyunsaturates
are < 10% of activity with the saturate. The presence of polyunsaturated
acyl CoA esters inhibits up to 70% the oxidation of palmitoyl CoA by intact
peroxisomes. Acyl CoA hydrolase activity is localized to peroxisomal
fractions prepared by density-gradient centrifugation. Hydrolytic activity
in these fractions is nearly twofold the activity of beta-oxidation.
Estimates for metabolic partitioning suggest that at least 50% of hepatic
beta-oxidation may be initiated by the peroxisomal compartment.
